K. Lundberg et al., INTERMEDIATE STEPS IN POSITIVE SELECTION - DIFFERENTIATION OF CD4-8+TCR(HI) THYMOCYTES(8(INT) TCR(INT) THYMOCYTES INTO CD4), The Journal of experimental medicine, 181(5), 1995, pp. 1643-1651
The differentiation potential of putative intermediates between CD4(+)
8(+) thymocytes and mature T cells has been examined. Such intermediat
e populations were sorted, in parallel with CD4(+)8(+) thymocytes, fro
m three types of C57BL/6 mice: major histocompatibility complex (MHC)
class II-deficient mice, mice transgenic for an alpha/beta T cell rece
ptor (TCR) restricted by class I MHC and normal mice. The sorted popul
ations were then transferred into the thymus of nonirradiated C57BL/Ka
mice differing in Thy 1 allotype, and the progeny of the transferred
cells were analyzed 2 d later. Surprisingly, with all three types of d
onor mice, a major proportion of the CD4(+)8(int)TCR(int)-derived prog
eny were found to be CD4(-)8(+)TCR(hi) cells, thus delineating a new a
lternative pathway for development of the CD8 lineage. In contrast, th
e transfer of CD4(int)8(+)TCR(int) thymocytes produced CD4(-)8(+)TCR(h
i) cells but no significant proportion of CD4(+)8(-)TCR(hi) cells, sug
gesting that there is no equivalent alternative pathway for the CD4 li
neage. The results negate some of the evidence for a stochastic/select
ive model of lineage commitment, and point to an asymmetry in the step
s leading to CD4(-)8(+) versus CD4(+)8(-) T cells.